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首页> 外文期刊>Neuroscience Letters: An International Multidisciplinary Journal Devoted to the Rapid Publication of Basic Research in the Brain Sciences >Systemically administered human bone marrow-derived mesenchymal stem home into peripheral organs but do not induce neuroprotective effects in the MCAo-mouse model for cerebral ischemia
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Systemically administered human bone marrow-derived mesenchymal stem home into peripheral organs but do not induce neuroprotective effects in the MCAo-mouse model for cerebral ischemia

机译:全身施用人骨髓来源的间充质干细胞进入周围器官,但在MCAo-小鼠脑缺血模型中不诱导神经保护作用

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摘要

Mesenchymal stem cells (MSC) from bone marrow induce neuroprotective effects and improve clinical symptoms in animal models for acute cerebral ischemia. So far only few data are available from the murine system. Moreover, no data exist regarding neuroprotective effects depending on the application route. Because most preclinical trials regarding restorative therapy in stroke are performed in mice, we aimed to investigate the neuroprotective capacities of human MSC (hMSC) in the middle cerebral artery occlusion (MCAo)-mouse model of cerebral ischemia. As systemic transplantation of MSC could provide a gentle therapeutic procedure for the (mostly elderly) stroke patients, we analyzed effects of this application at a clinically relevant time point. Bone marrow-derived hMSCs were administered intravenously 24. h after MCAo. Mortality and clinical outcome of the transplanted mice did not differ from PBS-treated controls. After 3 and 7 days hMSC were robustly detected in lung, spleen, kidney and intestine, but not in the brain. MRI measurements revealed no differences in infarct size in hMSC injected animals compared to controls. In the neurogenic subventricular zone and the dentate gyrus no significant increase of endogenous cell proliferation was detected following systemic hMSC transplantation. This data further prove the week neurogenic and neuroprotective effect and the limitations of systemically administered hMSCs in cerebral ischemia.
机译:骨髓间充质干细胞(MSC)可以诱导神经保护作用,并改善急性脑缺血动物模型的临床症状。到目前为止,鼠科系统只有很少的数据可用。而且,根据应用途径,没有关于神经保护作用的数据。因为大多数关于中风恢复性治疗的临床前试验都是在小鼠中进行的,所以我们旨在研究人MSC(hMSC)在大脑缺血的大脑中动脉闭塞(MCAo)-小鼠模型中的神经保护能力。由于MSC的全身移植可以为(大多数为老年)中风患者提供温和的治疗程序,因此我们在临床相关的时间点分析了该应用的效果。在MCAo后24小时静脉内施用源自骨髓的hMSC。移植小鼠的死亡率和临床结果与PBS处理的对照组没有差异。 3天和7天后,在肺,脾,肾和肠中检测到hMSC,但在脑中未检测到hMSC。 MRI测量显示与对照组相比,hMSC注射动物的梗死面积无差异。在系统性hMSC移植后,在神经源性脑室下区和齿状回中,未检测到内源性细胞增殖的显着增加。该数据进一步证明了一周的神经源性和神经保护作用以及全身给药的hMSC在脑缺血中的局限性。

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